肾内内皮素1、内皮素3和血管紧张素II表达在大鼠慢性环孢素A肾毒性中的作用。

C Ramírez, A Olmo, F O'Valle, M Masseroli, M Aguilar, M Gómez-Morales, F Revelles, M J García-Chicano, F Arrebola, M E Reguero, R G del Moral
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引用次数: 44

摘要

内皮素1 (Et1)在肾脏中广泛表达,与多种功能和向硬化发展的病理状况有关。内皮素3 (Et3)在肾脏水平上的功能尚存争议,但它可能通过作用于小管B型受体在水的重吸收中具有重要的调节功能。血管紧张素II最近被认为是环孢素A (CsA)诱导的间质纤维化进展的主要因素。我们在体内研究了这种关系,并分析了25 mg/kg/天CsA对Sprague-Dawley大鼠28和56天CsA毒性引起的修饰。采用免疫组织化学方法和分子分析方法研究Et1和Et3的表达,单独采用免疫组织化学方法测定肾内血管紧张素II的表达。经CsA处理的大鼠出现慢性肾毒性病变;半定量分析显示,时间的推移影响了这种病变的范围,导致肾小球总面积的减少。免疫组化结果显示,慢性CsA治疗诱导Et1和Et3在肾小管和肾小球水平适度分泌,治疗组血管紧张素II的局部表达比对照组更明显。此外,从CsA处理后28 d开始,preproEt3 mRNA水平显著升高(对照组0.07+/-0.11,CsA组0.48+/-0.11,p0.50, p0.50, p
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Role of intrarenal endothelin 1, endothelin 3, and angiotensin II expression in chronic cyclosporin A nephrotoxicity in rats.

Endothelin 1 (Et1) is widely expressed in the kidney and is related to several functions and to pathological conditions with progression towards sclerosis. The function of endothelin 3 (Et3) at the renal level is debatable, but it could have an important regulatory function in the reabsorption of water through its action on tubular type B receptors. Angiotensin II has recently been implicated as the principal factor responsible for the progression of interstitial fibrosis induced by cyclosporin A (CsA). We investigated this relationship in vivo and analyzed the modifications induced by CsA toxicity in Sprague-Dawley rats treated with 25 mg/kg/day of CsA for 28 and 56 days. Immunohistochemical methods and molecular analysis were used to study the expression of Et1 and Et3 and immunohistochemistry alone to determine the intrarenal expression of angiotensin II. Rats treated with CsA developed chronic nephrotoxicity lesions; semiquantitative analyses of hyaline arteriolopathy revealed that the passage of time affected the extent of this lesion and led to the diminution of the total glomerular area. Immunohistochemical results showed that chronic CsA treatment induced moderate secretion of Et1 and Et3 at tubular and glomerular levels and that the local expression of angiotensin II in the treatment groups was more evident than in control animals. Besides, the mRNA levels of preproEt3 showed a dramatic increase from 28 days after CsA treatment (control group 0.07+/-0.11 vs. CsA group 0.48+/-0.11, p<0.01), while the mRNA levels of preproEt1 increased from 56 days (control group 0.15+/-0.05 vs. CsA group 0.34+/-0.09, p< 0.05). At 28 days, renal lesions correlated strongly with the mRNA levels of Et3 (r>0.50, p<0.01). However, at 56 days, the key finding was the strong correlation of the most important analytical, histological, and immunohistochemical parameters of CsA nephrotoxicity with Et1 mRNA levels (r>0.50, p<0.01). These results support the hypothesis that the clinical and morphological phenomena linked with CsA nephrotoxicity are related to hypersecretion of endothelins and local expression of angiotensin II in the outer medulla and medullary rays; Et3 and angiotensin II are the first to act, followed subsequently by Et1.

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